The vitamin D receptor (VDR) is a nuclear hormone receptor that regulates cell proliferation, cell differentiation, and calcium homeostasis. The receptor is activated by vitamin D analogues that induce the disruption of VDR-corepressor binding and promote VDR-coactivator interactions. The interactions between VDR and coregulators are essential for VDR-mediated transcription. Small molecule inhibition of VDR-coregulator binding represents an alternative method to the traditional ligand-based approach in order to modulate the expression of VDR target genes. A high throughput fluorescence polarization screen that quantifies the inhibition of binding between VDR and a fluorescently labeled steroid receptor coactivator 2 peptide was applied to discover the new small molecule VDR-coactivator inhibitors, 3-indolylmethanamines. Structure-activity relationship studies with 3-indolylmethanamine analogues were used to determine their mode of VDR-binding and to produce the first VDR-selective and irreversible VDR-coactivator inhibitors with the ability to regulate the transcription of the human VDR target gene TRPV6.
Discovery of the first irreversible small molecule inhibitors of the interaction between the vitamin D receptor and coactivators.
发现了维生素 D 受体与辅激活剂相互作用的首个不可逆小分子抑制剂
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作者:Nandhikonda Premchendar, Lynt Wen Z, McCallum Megan M, Ara Tahniyath, Baranowski Athena M, Yuan Nina Y, Pearson Dana, Bikle Daniel D, Guy R Kiplin, Arnold Leggy A
| 期刊: | Journal of Medicinal Chemistry | 影响因子: | 6.800 |
| 时间: | 2012 | 起止号: | 2012 May 24; 55(10):4640-51 |
| doi: | 10.1021/jm300460c | 研究方向: | 信号转导 |
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